| Literature DB >> 34256129 |
Vaidehi Jobanputra1, Kazimierz O Wrzeszczynski2, Reinhard Buttner3, Carlos Caldas4, Edwin Cuppen5, Sean Grimmond6, Torsten Haferlach7, Charles Mullighan8, Anna Schuh9, Olivier Elemento10.
Abstract
Whole-genome sequencing either alone or in combination with whole-transcriptome sequencing has started to be used to analyze clinical tumor samples to improve diagnosis, provide risk stratification, and select patient-specific therapies. Compared with current genomic testing strategies, largely focused on small number of genes tested individually or targeted panels, whole-genome and transcriptome sequencing (WGTS) provides novel opportunities to identify and report a potentially much larger number of actionable alterations with diagnostic, prognostic, and/or predictive impact. Such alterations include point mutations, indels, copy- number aberrations and structural variants, but also germline variants, fusion genes, noncoding alterations and mutational signatures. Nevertheless, these comprehensive tests are accompanied by many challenges ranging from the extent and diversity of sequence alterations detected by these methods to the complexity and limited existing standardization in interpreting them. We describe the challenges of WGTS interpretation and the opportunities with comprehensive genomic testing.Entities:
Keywords: Clinical genomics; Data integration; Electronic medical records; Molecular tumor boards; Targeted therapy; Whole-genome sequencing; Whole-transcriptome sequencing
Mesh:
Year: 2021 PMID: 34256129 DOI: 10.1016/j.semcancer.2021.07.003
Source DB: PubMed Journal: Semin Cancer Biol ISSN: 1044-579X Impact factor: 17.012